Potent and selective oxytocin receptor agonists without disulfide bridges

Yusuke Adachi; Katsuya Sakimura; Yuji Shimizu; Masaharu Nakayama; Yasuko Terao; Takahiko Yano; Taiji Asami

doi:10.1016/j.bmcl.2017.04.030

Potent and selective oxytocin receptor agonists without disulfide bridges

Bioorg Med Chem Lett. 2017 Jun 1;27(11):2331-2335. doi: 10.1016/j.bmcl.2017.04.030. Epub 2017 Apr 12.

Authors

Yusuke Adachi¹, Katsuya Sakimura¹, Yuji Shimizu¹, Masaharu Nakayama¹, Yasuko Terao¹, Takahiko Yano¹, Taiji Asami²

Affiliations

¹ Pharmaceutical Research Division, Takeda Pharmaceutical Company, Ltd., Fujisawa 251-8555, Japan.
² Pharmaceutical Research Division, Takeda Pharmaceutical Company, Ltd., Fujisawa 251-8555, Japan. Electronic address: taiji.asami@takeda.com.

PMID: 28438540
DOI: 10.1016/j.bmcl.2017.04.030

Abstract

Oxytocin (OT) is a neuropeptide involved in a wide variety of physiological actions, both peripherally and centrally. Many human studies have revealed the potential of OT to treat autism spectrum disorders and schizophrenia. OT interacts with the OT receptor (OTR) as well as vasopressin 1a and 1b receptors (V_1aR, V_1bR) as an agonist, and agonistic activity for V_1aR and V_1bR may have a negative impact on the therapeutic effects of OTR agonism in the CNS. An OTR-selective agonistic peptide, FE 202767, in which the structural differences from OT are a sulfide bond instead of a disulfide bond, and N-alkylglycine replacement for Pro at position 7, was reported. However, the effects of amino acid substitutions in OT have not been comprehensively investigated to compare OTR, V_1aR, and V_1bR activities. This led us to obtain a new OTR-selective analog by comprehensive amino acid substitutions of OT and replacement of the disulfide bond. A systematic amino acid scanning (Ala, Leu, Phe, Ser, Glu, or Arg) of desamino OT (dOT) at positions 2, 3, 4, 5, 7, and 8 revealed the tolerability for the substitution at positions 7 and 8. Further detailed study showed that trans-4-hydroxyproline (trans-Hyp) at position 7 and γ-methylleucine [Leu(Me)] at position 8 were markedly effective for improving receptor selectivity without decreasing the potency at the OTR. Subsequently, a combination of these amino acid substitutions with the replacement of the disulfide bond of dOT analogs with a sulfide bond (carba analog) or an amide bond (lactam analog) yielded several promising analogs, including carba-1-[trans-Hyp⁷,Leu(Me)⁸]dOT (14) with a higher potency (7.2pM) at OTR than that of OT and marked selectivity (>10,000-fold) over V_1aR and V_1bR. Hence, we investigated comprehensive modification of OT and obtained new OT analogs that exhibited high potency at OTR with marked selectivity. These OTR-selective agonists could be useful to investigate OTR-mediated effects on psychiatric disorders.

Keywords: Agonist; Oxytocin; Peptide; Vasopressin.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
CHO Cells
Cricetulus
Disulfides / chemistry*
Humans
Receptors, Oxytocin / agonists*

Substances

Disulfides
Receptors, Oxytocin